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• W4362559637 endingPage "6707" @default.
• W4362559637 startingPage "6707" @default.
• W4362559637 abstract "Inflammation is pathogenic to skin diseases, including atopic dermatitis (AD) and eczema. Treatment for AD remains mostly symptomatic with newer but costly options, tainted with adverse side effects. There is an unmet need for safe therapeutic and preventative strategies for AD. Resveratrol (R) is a natural compound known for its anti-inflammatory properties. However, animal and human R studies have yielded contrasting results. Mast cells (MCs) are innate immune skin-resident cells that initiate the development of inflammation and progression to overt disease. R’s effects on MCs are also controversial. Using a human-like mouse model of AD development consisting of a single topical application of antigen ovalbumin (O) for 7 days, we previously established that the activation of MCs by a bioactive sphingolipid metabolite sphingosine-1-phosphate (S1P) initiated substantial skin remodeling compared to controls. Here, we show that daily R application normalized O-mediated epidermal thickening, ameliorated cell infiltration, and inhibited skin MC activation and chemokine expression. We unraveled R’s multiple mechanisms of action, including decreased activation of the S1P-producing enzyme, sphingosine kinase 1 (SphK1), and of transcription factors Signal Transducer and Activator of Transcription 3 (Stat3) and NF-κBp65, involved in chemokine production. Thus, R may be poised for protection against MC-driven pathogenic skin inflammation." @default.
• W4362559637 created "2023-04-06" @default.
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• W4362559637 date "2023-04-04" @default.
• W4362559637 modified "2023-10-05" @default.
• W4362559637 title "Resveratrol Protects against Skin Inflammation through Inhibition of Mast Cell, Sphingosine Kinase-1, Stat3 and NF-κB p65 Signaling Activation in Mice" @default.
• W4362559637 cites W1548494899 @default.
• W4362559637 cites W1976547449 @default.
• W4362559637 cites W1978707192 @default.
• W4362559637 cites W1978889258 @default.
• W4362559637 cites W1982386486 @default.
• W4362559637 cites W1985668252 @default.
• W4362559637 cites W1990636742 @default.
• W4362559637 cites W1992820573 @default.
• W4362559637 cites W1994190235 @default.
• W4362559637 cites W2004171945 @default.
• W4362559637 cites W2009251019 @default.
• W4362559637 cites W2011119433 @default.
• W4362559637 cites W2015202977 @default.
• W4362559637 cites W2018780332 @default.
• W4362559637 cites W2020118676 @default.
• W4362559637 cites W2020671379 @default.
• W4362559637 cites W2031449170 @default.
• W4362559637 cites W2033825102 @default.
• W4362559637 cites W2036781144 @default.
• W4362559637 cites W2039603982 @default.
• W4362559637 cites W2066439088 @default.
• W4362559637 cites W2070124969 @default.
• W4362559637 cites W2089635060 @default.
• W4362559637 cites W2092576605 @default.
• W4362559637 cites W2096279219 @default.
• W4362559637 cites W2101046775 @default.
• W4362559637 cites W2106301295 @default.
• W4362559637 cites W2119536609 @default.
• W4362559637 cites W2122044177 @default.
• W4362559637 cites W2132805096 @default.
• W4362559637 cites W2133470606 @default.
• W4362559637 cites W2146302565 @default.
• W4362559637 cites W2151089147 @default.
• W4362559637 cites W2154360165 @default.
• W4362559637 cites W2161269202 @default.
• W4362559637 cites W2164929014 @default.
• W4362559637 cites W2167005174 @default.
• W4362559637 cites W2172640301 @default.
• W4362559637 cites W2235386298 @default.
• W4362559637 cites W2238227876 @default.
• W4362559637 cites W2396659319 @default.
• W4362559637 cites W2431476183 @default.
• W4362559637 cites W2515620899 @default.
• W4362559637 cites W2603291804 @default.
• W4362559637 cites W2754548275 @default.
• W4362559637 cites W2781686976 @default.
• W4362559637 cites W2789447956 @default.
• W4362559637 cites W2800613191 @default.
• W4362559637 cites W2807330238 @default.
• W4362559637 cites W2886886286 @default.
• W4362559637 cites W2889245387 @default.
• W4362559637 cites W2899071879 @default.
• W4362559637 cites W2902539416 @default.
• W4362559637 cites W2905681354 @default.
• W4362559637 cites W2905767886 @default.
• W4362559637 cites W2928939598 @default.
• W4362559637 cites W3009230457 @default.
• W4362559637 cites W3013908850 @default.
• W4362559637 cites W3019563208 @default.
• W4362559637 cites W3099504599 @default.
• W4362559637 cites W3169904987 @default.
• W4362559637 cites W3183991840 @default.
• W4362559637 cites W3187038212 @default.
• W4362559637 cites W3206698011 @default.
• W4362559637 cites W4206927880 @default.
• W4362559637 cites W4213355780 @default.
• W4362559637 cites W4220935032 @default.
• W4362559637 cites W4232712261 @default.
• W4362559637 cites W4281647810 @default.
• W4362559637 cites W4282042895 @default.
• W4362559637 cites W4285011088 @default.
• W4362559637 cites W4286632619 @default.
• W4362559637 cites W4303958873 @default.
• W4362559637 cites W4311089308 @default.
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• W4362559637 doi "https://doi.org/10.3390/ijms24076707" @default.
• W4362559637 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/37047680" @default.
• W4362559637 hasPublicationYear "2023" @default.
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